Efficacy, safety and pharmacokinetics of Unecritinib (TQ-B3101) for patients with ROS1 positive advanced non-small cell lung cancer: a Phase I/II Trial

This phase I/II trial characterized the tolerability, safety, and antitumor activities of unecritinib, a novel derivative of crizotinib and a multi-tyrosine kinase inhibitor targeting ROS1, ALK, and c-MET, in advanced tumors and ROS1 inhibitor-naive advanced or metastatic non-small cell lung cancer (NSCLC) harboring ROS1 rearrangements. Eligible patients received unecritinib 100, 200, and 300 mg QD, and 200, 250, 300, and 350 mg BID in a 3 + 3 design during dose escalation and 300 and 350 mg BID during expansion. Phase II trial patients received unecritinib 300 mg BID in continuous 28-day cycles until disease progression or unacceptable toxicity. The primary endpoint was the objective response rate (ORR) per independent review committee (IRC). Key secondary endpoints included intracranial ORR and safety. The ORR of 36 efficacy evaluable patients in the phase I trial was 63.9% (95% CI 46.2%, 79.2%). In the phase II trial, 111 eligible patients in the main study cohort received unecritinib. The ORR per IRC was 80.2% (95% CI 71.5%, 87.1%) and the median progression-free survival (PFS) per IRC was 16.5 months (95% CI 10.2, 27.0). Additionally, 46.9% of the patients who received recommended phase II dose of 300 mg BID experienced grade 3 or higher treatment-related adverse events. Treatment-related ocular disorders and neurotoxicity occurred in 28.1% and 34.4% of patients, respectively, but none was grade 3 or higher. Unecritinib is efficacious and safe for ROS1 inhibitor-naive patients with ROS1-positive advanced NSCLC, particularly patients with brain metastases at baseline, strongly supporting that unecritinib should become one of the standards of care for ROS1-positive NSCLC. ClinicalTrials.gov identifier: NCT03019276 and NCT03972189.


INTRODUCITON
Lung cancer remains the leading cause of cancer death globally, accounting for approximately one in five (18.0%) of the total cancer deaths, 1 and is expected to be the principal cause of death in both sexes in China and the USA in 2022. 2 Recent remarkable advances in molecular targeted therapies have significantly extended the survival of patients with lung cancer harboring actionable mutations including EGFR exon 19 deletion and L858R mutations, and ALK and ROS1 rearrangements. [3][4][5][6][7] The ROS1 oncogene, which is located on chromosome 6 (6q22), encodes protooncogene receptor tyrosine kinase ROS1. The kinase is composed of an intracellular C-terminus containing the kinase domain, a single transmembrane domain, and an extracellular Nterminal domain 8 and is constitutively activated by fusion partner proteins as a result of chromosomal rearrangements that occur in approximately 1% to 2% of patients with non-small cell lung cancer (NSCLC). [8][9][10] Among diverse ROS1 fusions, CD74 is the most frequent ROS1 fusion partner, and CD74-ROS1 fusion is present in~44% of NSCLC cases with ROS1 rearrangements. 9 Intriguingly, we have previously noted that NSCLC patients carrying CD74-ROS1 fusion are more likely to develop brain metastases. 11 Targeted therapies are well established for NSCLC with ALK and ROS1 rearrangements that lead to constitutive kinase activity of ALK or ROS1. 6 Crizotinib, an ALK and ROS1 tyrosine kinase inhibitor (TKI), has become not only one of the standards of care for ALK-positive but also the preferred drug for ROS1rearranged NSCLC patients. 12 Several pivotal trials, including the METROS trial, 13 the PROFILE 1001 study 14 and the OO 12-01 study, 15 have demonstrated that crizotinib elicits a durable response and extends the progressionfree survival (PFS) of patients with ROS1-rearranged advanced NSCLC, establishing ROS1 as a valid therapeutic target in ROS1rearranged lung cancers. However, despite significant improvement in the objective response rate (ORR) and survival outcome of ROS1-rearranged NSCLC patients, there are concerning treatmentrelated adverse events (TRAEs) such as prominent gastrointestinal disturbances and ocular toxicities with crizotinib 12,16 and neurotoxicity with entrectinib. 17 Unecritinib (TQ-B3101), a multi-TKI targeting ROS1, ALK, and c-MET, is a derivative of crizotinib via structural modification of the pyridine ring. Our in vitro study showed that similar to crizotinib, unecritinib inhibited AKT phosphorylation and its downstream signaling molecules ERK1/2 (extracellular signalregulated protein kinases 1 and 2) ( Supplementary Fig. S1). Furthermore, unecritinib had an IC 50 of 142.7 nM and an IC 90 of 821.3 nM while unecritinib M had an IC 50 of 0.8 nM and an IC 90 of 6.2 nM for wildtype ROS1. Unecritinib also displayed notable growth inhibitory effects on several cancer cell lines carrying ALK rearrangements or mutations or overexpressing c-MET, with an IC 50 of 180 to 378.9 nm for lung cancer cells and an IC 50 of 23.5 nm for gastric cancer cells overexpressing c-MET. The IC 50 of growth inhibition by unecritinib is comparable to that by crizotinib (Supplementary Table S1).
Meanwhile, our preclinical studies showed a greater bioavailability of unecritinib than crizotinib in beagles (data not published). In mouse xenografts bearing human lung adenocarcinoma NCI-H3122 cells, unecritinib showed greater tumor growth inhibition than crizotinib, which may be explained by higher tumor tissue exposure to unecritinib vs. crizotinib (data not published). Notably, unecritinib M, the metabolite of unecritinib, had a considerably lower AUC ocular tissue /AUC plasma than crizotinib in rats (data not published). The remarkably smaller distribution of unecritinib M in the ocular tissues suggests a lower risk of ocular toxicities. Indeed, no apparent ocular toxicities were observed in rats and beagles receiving unecritinib for 4 weeks (rats 135 mg/kg; beagles 81 mg/kg) (data not published).
In this phase I/II study, we aimed to characterize the tolerability, safety, and antitumor activities of unecritinib in ROS1 inhibitor- EZR-ROS1 and SLC34A2-ROS1 naive patients with ROS1-rearranged advanced NSCLC and other selected advanced solid tumors who had failed standard chemotherapy. As CD74 is the most frequent ROS1 fusion partner and CD74-ROS1 fusion is present in~44% of NSCLC cases with ROS1 rearrangements, 18,19 we also carried out a prespecified analysis of the efficacy of unecritinib for NSCLC cases with CD74-ROS1 fusion.

Patient characteristics
The phase I/II trial was conducted between July 12, 2017, and March 2, 2021, and the cutoff date for this analysis was December 20, 2021. Patient demographic, baseline, and prior treatment characteristics are described in Table 1 and the study flowcharts are shown in Supplementary Fig. S2. Twenty patients were enrolled in the dose escalation portion and 19 patients in the dose expanse portion of the phase I trial. Two of them (5.1%) had stage III tumors and 37 (94.9%) had stage IV tumors, and 61.5% received prior chemotherapy. One hundred sixty patients were screened for eligibility for the phase II trial and 113 patients were eligible and received unecritinib, including 2 patients in the exploratory study cohort and 111 patients in the main study cohort. In the main study cohort, 103 patients (92.8%) had stage IV NSCLC. Thirty-three patients (29.7%) had brain metastasis and 15 (13.5%) had liver metastasis. Forty-eight patients (43.2%) received prior chemotherapy. Forty patients with ROS1 rearrangement detected by AmoyDx assay at the central laboratory subsequently underwent central testing by NGS. The concordance rate was 100% between the Amoydx assay and central NGS testing (excluding samples that failed quality control). Twenty-seven patients (67.5%) had CD74-ROS1 fusion. Five patients (12.5%) had SDC4-ROS1 fusion, and 3 (7.5%) had SLC34A2-ROS1 fusion. In addition, EZR-ROS1 and TPM3-ROS1 fusion was each present in 1 patient (2.5%). Furthermore, one patient carried both EZR-ROS1 and TGFBR1-ROS1 fusions and another carried both EZR-ROS1 and SLC34A2-ROS1 fusions. ROS1 fusion partners were indeterminate in 71 patients who did not undergo NGS. The fusion as detected by AmoyDx assay and the patient could carry any one of the fusions as the assay does not report these three fusions (TPM3/ LRIG3/GOPC) individually

Safety
The safety population was composed of 128 patients, including three patients who received unecritinib 300 mg BID during dose escalation, 12 patients who received unecritinib 300 mg BID during dose expansion, and 113 patients from the phase 2 trial. Data on gene mutations were available from six patients from the phase 1 trial, including 3 cases who had ALK fusion, 2 cases who had unspecified ALK mutations, 1 case with unspecified ROS1 mutation. All 113 patients from the phase 2 trial had ROS1 fusions.
No dose-limiting toxicities (DLTs) were observed in the doseescalation portion of the phase I trial. Patients receiving unecritinib 300 mg BID reported lower rates of grade 3 or higher adverse events (AEs) and treatment-emergent AEs leading to dose reductions or interruptions than those receiving unecritinib 350 mg BID (Supplementary Table S2). Taking into consideration the results of subsequent efficacy analysis, we chose oral unecritinib 350 mg BID as the maximum-tolerated dose (MTD) and unecritinib 300 mg BID as the recommended phase II dose (RP2D) to provide a safe dosing regimen without jeopardizing the efficacy of unecritinib.
Grade 3 or higher TRAEs occurred in 41.0% of the patients in the phase I trial and 46.9% of the patients who received unecritinib 300 mg BID in both trials (Supplementary Tables S2 and S3). TRAEs led to dose reductions in 17.2% and dosing interruptions in 37.5% of the patients in all patients who received unecritinib 300 mg BID. Three patients (2.3%) discontinued unecritinib due to TRAEs. Among 128 patients who received RP2D 300 mg BID in both trials, the most frequently reported grade 3 or 4 TRAEs were reduced neutrophil count (25.8%), elevated alanine aminotransferase (7.8%), and reduced leukocyte count (6.3%) ( Table 2). Reduced neutrophil count led to treatment interruptions in 26 cases (20.3%), but no treatment discontinuation. Treatment-related ocular disorders (cluster term) were reported in 28.1% of the patients, but none were grade 3 or higher (Supplementary Table  4). Furthermore, 34.4% of the patients had neurotoxicity (cluster term), and none were grade 3 or higher. TRAEs were manageable through dose reductions or interruptions and supportive therapy. No treatment-related death occurred in either trial. In addition, 4 patients in the phase II trial received prior PD-1/PD-L1 inhibitor therapy. They experienced a total of 88 any grade TRAEs, all of which were grade 1 or 2 except grade 3 elevated alanine aminotransferase in 1 patient.

Pharmacokinetics
Unecritinib was rapidly absorbed regardless of doses or dosing schedule and reached peak plasma concentration in 30-60 min. Meanwhile, plasma unecritinib M concentrations peaked between 2 and 4 h after dosing ( Fig. 1 and Supplementary Fig.  S3). The levels of systemic exposure to unecritinib and unecritinib M (C max and AUC 0-t ) increased as the dose level increased from 100 to 200 mg (single oral administration) and from 100 to 300 mg QD (multiple once-daily oral administrations). The dose proportionality was inconclusive for multiple twice daily oral administrations. Unecritinib had a seemingly dose-independent and rather brief T 1/2 after single or multiple administrations. The short T 1/2 caused no significant plasma accumulation of unecritinib over time, with a geometric mean Rac between 0.8 and 1 at the steady state after multiple twicedaily oral administrations at 200-350 mg. Though the geometric mean Rac ranged between 0.8 and 1.5 at the steady state after multiple once-daily oral administrations at 100, 200, and 300 mg, it was dose independent. Notably, the metabolite of unecritinib had a considerably longer T 1/2 (between 4.6 and 69.9 h) after single or multiple administrations, which contributed to plasma accumulation of unecritinib M, with a geometric mean Rac between 3.6 and 6.0 at the steady state after multiple twice daily oral administrations at 200-350 mg. Overall, CL/F of unecritinib M declined over time after multiple twice-daily oral administrations at 200-350 mg. At the data cutoff, 53 patients were still receiving unecritinib. Of the 113 patients who received unecritinib, 2 patients in the exploratory study cohort were excluded from the efficacy analysis. One of the 111 efficacy evaluable patients attained CR and 88 of them achieved PR, with an ORR of 80.2% (95% CI 71.5%, 87.1%). Furthermore, 9 patients had SD, and the DCR was 88.3% (95% CI 80.8%, 93.6%). Eleven patients had PD. One hundred and nine patients experienced a reduction from baseline in target lesion size (Fig. 2b). The median DOR was 20.3 months (95% CI 11.0, 26.1) ( Table 3). Forty-eight PFS events had occurred and the median PFS was 16.5 months (95% CI 10.2, 27.0) (Fig. 2d). The 6-month PFS rate reached 83.2% (95% CI 74.6%, 89.0%) and the 12-month PFS rate 53.8% (95% CI 42.7%, 63.6%).

DISCUSSION
Recent remarkable advances in molecular targeted therapies for advanced NSCLC harboring mutations such as ALK and ROS1 rearrangement have extended the survival of these patients. [3][4][5][6]20 However, safety concerns such as ocular toxicities with crizotinib. 12,16 and neurotoxicity with entrectinib. 17 have emerged, highlighting the need for the development of effective and safer molecular targeted therapeutic agents. We developed a novel TKI, unecritinib, with favorable pharmacokinetics characteristics and promising antitumor activities, which, at the same time, avoided or lessened the special toxicities of crizotinib and entrectinib. Our preclinical evidence indicates that this novel multi-kinase inhibitor of ROS1, ALK and c-MET has a greater bioavailability than crizotinib, and unecritinib M has a 200-fold lower distribution in ocular tissues than crizotinib. As far as we know, this is the largest trial of ROS-1 positive tumors harboring ROS1 rearrangements showing that unecritinib had an acceptable toxicity profile, with lower rates of and no grade 3 or higher ocular toxicities and neurotoxicities, and elicited a durable response, with more than half (53.8%) of the patients being progression-free at 12 months. These findings demonstrate that unecritinib is safe and has promising activities against advanced NSCLC harboring ROS1 rearrangement.
In this trial, unecritinib demonstrated promising antitumor activities in advanced NSCLC patients with ROS1 rearrangement. Notably, unecritinib achieved an ORR by IRC of 80.2% while the ORR by IRC was 71.7% for crizotinib in the OO 12-01 study of East Asians with ROS1-positive advanced NSCLC 15 and 67.1% for entrectinib in the integrated analysis of data from the STARTRK-1 and −2 and ALKA-372-001 21 trials. The DCR reached 88.3% with unecritinib and is comparable to that of crizotinib (88.2%) 15 and higher than that (75.8%) of entrectinib. 21 The median PFS was 16.5 months in the current trial and 15.9 months with crizotinib 15 and 15.7 months with entrectinib in the integrated analysis of data from the STARTRK-1 and -2 and ALKA-372-001 21 trials. The high efficacy of unecritinib could be at least partially attributed to its high levels in the tumor tissues, as shown in our preclinical studies (data not published).
Previous studies showed that NSCLC patients with ROS1 fusions are more predisposed to brain metastases 22 ; 20-50% of NSCLC patients have brain metastases, 22 and CNS is the site of initial progression in approximately half of ROS1 fusion-positive NSCLC patients treated with crizotinib, 23 highlighting the importance of CNS activity for ROS1 TKIs. There are no preclinical data on the comparison of the intracranial efficacy of unecritinib versus other ROS1 inhibitors. 24 In the current study, the ORR of the patients who had brain metastases at baseline was 72.7% while that of entrectinib was 62.5%. In addition, unecritinib achieved an intracranial ORR of 72.7% per IRC among patients with baseline intracranial target lesions, which is largely comparable to that attained with entrectinib (79.2%) in the integrated analysis of data from the STARTRK-1 and -2 and ALKA-372-001 21 trials. Notably, 46.4% of these patients in the integrated analysis had received radiotherapy for brain metastases, including 20 patients who received radiotherapy within the preceding 6 months and 26 patients who received or did not receive radiotherapy before the preceding 6 months. The intracranial ORR was 60% for those who had received radiotherapy within the preceding 6 months versus 46.2% for those who had not. Meanwhile, the intracranial PFS was 16.1 months for those who had received radiotherapy within the preceding 6 months versus 8.8 months for those who had not. Only 9 (8.1%) of our patients had received radiotherapy and 9.1% of the patients with baseline brain lesions had received radiotherapy. Meanwhile, ceritinib had a low intracranial ORR (29%) in NSCLC with ROS1 rearrangements. 25 Intracranial response to crizotinib was not assessed in the phase II OO 12-01 study of East Asians with ROS1-positive advanced NSCLC. 15 and the intracranial ORR was 33% (2/6) with crizotinib in the phase II METROS trial. 13 In addition, the median intracranial PFS reached 10.1 months in our patients with baseline intracranial target lesions versus 12.0 months with entrectinib in patients with measurable central nervous system lesions at baseline. 21 Accurate delineation of targetable oncogenic alterations is critical to the targeted therapies for NSCLC 21 and testing of all nonsquamous NSCLC for therapy-predictive biomarkers is recommended in clinical practice guidelines. 26 Our previous study showed that NSCLC patients with different ROS1 fusions responded differently to crizotinib therapy. 22 Among diverse ROS1 fusions, CD74 is the most frequent ROS1 fusion partner and CD74-ROS1 fusion is present iñ 44% of NSCLC cases with ROS1 rearrangements. 18,19 In this trial, about two-thirds of the NSCLC patients (67.5%) who had undergone central NGS testing had CD74-ROS1 fusion. Currently, it remains inconclusive whether TKI is efficacious for NSCLC harboring CD74- ROS1 fusions. In the PROFILE 1001 trial, crizotinib efficacy was independent of ROS1 translocation type. 14 A retrospective analysis showed that patients whose tumor harboring CD74-ROS1 had a significantly shorter median PFS with first-line crizotinib than those harboring non-CD74-ROS1 fusions 27 (17.0 months vs. 21.0 months; P = 0.008). Reduced efficacy of crizotinib in CD74-ROS1-positive patients was also noted by other investigators. 12,22 The ORR with entrectinib for those with CD74-ROS1 fusions was 72.9%, which is higher than that (67.1%) of the overall patient populations. 21 In the current trial, unecritinib attained an ORR of 88.9% in patients with CD74-ROS1 rearrangements, and the median PFS of these patients doubled that of patients without CD74-ROS1 rearrangements (21.2 vs. 10.1 months). To our knowledge, this is the first time that ROS1-TKI has been found to have a greater ORR and longer PFS in a large sample of patients with CD74-ROS1 rearrangements in a prospective clinical study. The safety profile of unecritinib is overall consistent with that of other ROS1 inhibitors. The rate of drug dose interruptions due to TRAEs was 37.5% in the patients who received unecritinib 300 mg BID, which is higher than that (22.8%) of crizotinib. 15 However, the proportion of patients who discontinued treatment due to TRAEs is low in these patients (2.3%) and comparable to that of crizotinib. 12 Reduced neutrophil count was the most frequent TRAE in this study, occurring in 25.8% of the patients, compared to 12% with crizotinib. 12 Reduced neutrophil count contributed to treatment interruptions in this trial, but it was manageable through dose reductions or interruptions and supportive therapy, which may explain the similar rate of treatment discontinuations of unecritinib and crizotinib. Among 128 patients who received unecritinib 300 mg BID, the other most frequently reported grade 3 or 4 TRAEs included elevated alanine aminotransferase (7.8%), and reduced leukocyte count (6.3%), which are common AEs that are also reported with other ROS1 TKIs. The TRK family of kinases are implicated in CNS homeostasis and inhibition of these kinases may lead to CNS symptoms such as dizziness and dysgeusia. 28 Dizziness occurred in 10.9% and dysgeusia in 13.3% of our patients receiving unecritinib 300 mg BID, but neither was grade 3 or higher. These CNS abnormalities were also reported in NSCLC patients treated with crizotinib (dizziness 16%; dysgeusia 18%) 12 and entrectinib (dizziness 34.8%; dysgeusia 43.4%). 21 Ophthalmological AEs are unique AEs that were reported in a high proportion of NSCLC patients treated with crizotinib (82%) 12 and also occurred in patients treated with other ROS1 inhibitors including brigatinib, 29 entrectinib, 30 and lorlatinib. 18 As expected, ophthalmological AEs including visual impairment and blurred vision occurred in 36 patients (28.1%) in the current trial. This low rate of ophthalmological AEs might be at least partially due to the notably smaller distribution of unecritinib metabolite in ocular tissues than that of crizotinib, as shown in our preclinical studies (data not published). In addition, though the rate of any grade elevated AST (73.4%) and elevated ALT (71.9%) is higher with unecritinib than that reported for crizotinib (22% and 14%, respectively), 4 the rate of grade III or higher elevated AST (3.9%) and ALT (7.8%) is largely comparable to crizotinib (2% and 4%, respectively). A previous pharmacokinetics analysis of quantifiable unecritinib and unecritinib M data from 40 subjects after oral administration of unecritinib showed that unecritinib pharmacokinetics could be explained by a 1-compartment model with first-order absorption and elimination for unecritinib coupled with a 2-compartment model with time-dependent clearance for the metabolite. 31 Our pharmacokinetics analysis found that the AUC 0 -t of unecritinib increased in a dose-proportional manner following rapid intestinal absorption of unecritinib BID from 200 to 350 mg. However, there was no apparent accumulation of unecritinib with unecritinib BID. The metabolite unecritinib M had considerable plasma accumulation at the steady state after multiple twice-daily oral administrations at 200-350 mg. Unecritinib is not a next-generation ROS1 inhibitor that could overcome ROS1 resistance mutations. Novel nextgeneration TKIs such as repotrectinib which has highly potent activities against ROS1, TRKA-C, and ALK could target on-target kinase domain mutations, which are a major mechanism of acquired resistance. 32 In the early-stage TRIDENT-1 trial, repotrectinib demonstrated potent activities in ROS1 rearranged NSCLC with solvent-front mutations. 33 Taletrectinib, a novel ROS1 and pan-NTRK TKI, has demonstrated preclinical activities against ROS1 G2032R solvent-front mutation and also shown meaningful clinical antitumor activities against advanced crizotinib-refractory ROS1 + NSCLC. 34 The 4 th generation TKI NVL-655 with activities against a variety of ALK mutations is under active development. 35 These novel TKIs could offer potentially effective treatment for NSCLC with solvent-front mutations including ALK G1202R , ROS1 G2032R or ROS1 D2033N , TRKA G595R , and TRKC G623R . Two patients in our study received prior crizotinib and achieved PR. It is of intrigue and clinical relevance to learn whether unecritinib could also target ROS1 resistance mutations in advanced NSCLC, the answer to which, however, requires validation in future clinical trials with a larger target population.
Overall, this study demonstrated that unecritinib had an acceptable safety profile and established the clinical benefit of unecritinib for ROS1 inhibitor-naive patients with ROS1-positive advanced NSCLC and other selected advanced solid tumors who had failed prior chemotherapy. Notably, unecritinib was more effective in CD74-ROS1 rearrangements NSCLC patients. Given that the CNS is a common site of metastases and a frequent site of disease progression in advanced NSCLC, unecritinib led to durable intracranial tumor responses, reflecting its potent intracranial activities. The findings strongly support that unecritinib should become one of the standards of care for NSCLC harboring ROS1 rearrangements, particularly those patients with baseline brain metastases or CD74-ROS1 fusions, and further clinical development of unecritinib for NSCLC with ALK rearrangement is warranted. Screening criteria This phase I/II trial enrolled adult patients with histologically confirmed advanced tumors (phase I) or locally advanced or metastatic NSCLC with ROS1 rearrangements (phase II). ROS1 rearrangements were determined using a reverse transcriptionpolymerase chain reaction (RT-PCR) AmoyDx assay. 15 (Amoy Diagnostics, Xiamen, China) in the main study cohort of the phase II trial. Furthermore, ROS1 fusions detected at the central laboratory underwent next-generation sequencing (NGS) for further comparison of efficacy for patients with CD74-ROS1 fusions and those with non-CD74-ROS1 fusions if there were enough tissue. NGS was performed on the NextSeq CN500 platform (Berry Genomics Co., Ltd) at a central laboratory using the HANDLE Classic NGS Panel (Amoy Diagnostics). Patients who were positive for ROS1 fusions other than those included in the AmoyDx assays as detected by fluorescent in situ hybridization (FISH) or NGS and those who progressed on crizotinib were categorized into the exploratory study cohort of the phase II trial. Other eligibility criteria were no more than two prior chemotherapy regimens, at least one radiologically confirmed measurable target lesion per Response Evaluation Criteria in Solid Tumors (RECIST) version 1.1, and an Eastern Cooperative Oncology Group (ECOG) performance status (PS) of 0-1. Prior therapy with crizotinib or other ROS1 inhibitors was not permitted in the main study cohort. Additional eligibility criteria are provided in the study protocol.

Study design and treatment
In the phase I trial, the MTD and the RP2D were determined using a dose-escalation strategy with a 3 + 3 design using a modified Fibonacci scheme, with preferential enrollment of ALK and ROS1rearranged NSCLC patients. In the phase II trial, all patients harboring ROS1 rearrangement received the RP2D of unecritinib 300 mg twice daily (BID) orally in continuous 28-day cycles until disease progression or development of unacceptable toxicity. The primary endpoints for phase I trial were to determine the safety, tolerability, DLTs, MTD, and pharmacokinetics of unecritinib. The primary endpoint of the phase II trial was ORR per the independent review committee (IRC). Secondary endpoints included the antitumor activities of unecritinib in ALK-and ROS1-rearranged advanced lung cancer patients for phase I and duration of response (DOR), disease control rate (DCR), PFS, intracranial ORR, intracranial DOR, intracranial time to progression (TTP), intracranial PFS, overall survival and safety for phase II.
Dose modification was allowed for grade 3 or higher adverse events (AEs) per the National Cancer Institute Common Terminology Criteria for AEs (NCI-CTC AE) version 5.0, with two levels of dose reduction, from 300 mg BID to 250 mg BID and from 250 mg BID to 200 mg BID. If more than two dose levels need to be reduced, the study treatment was terminated.
The trial protocols were approved by the independent ethics committee at each site and complied with the International Ethical Guidelines for Biomedical Research Involving Human Subjects. The studies were conducted according to Good Clinical Practice guidelines and the Declaration of Helsinki. All patients provided written informed consent prior to any trial activities.

Assessments
Tumor responses were evaluated by investigators and IRC per RECIST v1.1 using computed tomography (CT) or magnetic resonance imaging (MRI) within 2 weeks of study entry, at 6 weeks post-treatment, and once every two cycles thereafter. Complete response (CR), partial response (PR), and stable disease (SD) had to be confirmed with a repeat scan after at least 6 weeks. The response of intracranial disease was evaluated radiologically per Response Assessment in Neuro-Oncology Brain Metastases (RANO-BM). AEs were evaluated using NCI-CTC AE version 5.0.
Pharmacokinetic assessments Blood samples for pharmacokinetics analyses were collected predose on days 1, 7, 14, 21, and 28, and 30 min, 1, 2, 4, 6, 10, and 12 h postdose on days 1 and 28. The concentrations of unecritinib and unecritinib M were measured by tandem mass spectrometry hyphenated to liquid chromatography separation systems (HPLC-MS/MS). The pharmacokinetics parameters were calculated by non-compartmental analysis (NCA) model using WinNonLin ® v 6.4 (Certara, Princeton, NJ, USA) and included C max and time to reach C max (T max ), minimum and average steady-state concentration [C SS(min) and C ss-av ], the area under the steady-state plasma concentration-time curve (AUC ss ), terminal elimination half-life (T 1/2 ) and degree of fluctuation.

Statistical analysis
Based on the phase II OO 12-01 study, 15 an ORR of 50% as the lower limit of two-sided 95% CI was required to demonstrate the efficacy of unecritinib. The statistical power (1−β) to demonstrate efficacy based on this threshold was 85%. For a targeted ORR of 65%, with one-sided α of 0.025, 94 evaluable patients with ROS1rearranged NSCLC were required for the main study cohort of the phase II trial. Assuming a drop-off rate of 15%, the maximum estimated target sample size was 111.
The Full Analysis Set (FAS) included all enrolled patients who had received at least one dose of unecritinib except for the patients enrolled into the exploratory study cohort, and the Per Protocol Set (PPS) included all enrolled patients who had received at least one cycle of treatment, with at least one radiological evaluation, good compliance, and no major study protocol violations. The pharmacokinetics concentration set included all enrolled patients who had received at least one dose of unecritinib and had one post-treatment measurement of plasma concentration of unecritinib. The pharmacokinetics parameter set includes all enrolled patients who had received at least one dose of unecritinib and had at least one valid pharmacokinetic parameter data. The safety set included all enrolled patients who had received at least one dose of unecritinib. No imputation was done for missing data. We estimated 95% CIs using the conventional Wald method for ORR and the Clopper-Pearson method for DCR and intracranial ORR. ORR and its 95% CI were presented graphically using forest plots. Kaplan-Meier methods were used to determine medians and 95% CIs for DOR, PFS, intracranial DOR, intracranial TTP and intracranial PFS. AEs were mainly analyzed using descriptive statistics. Statistical analyses were undertaken using the SAS software package, version 9.4 M5 (SAS Institute Inc., Cary, NC). All tests were two-tailed with a level of significance set at P ≤ 0.05.

DATA AVAILABILITY
The datasets used and/or analyzed during the current study are available from the corresponding author on reasonable request.